因 XDH 基因同源缺失导致的遗传性黄嘌呤尿继发肾衰竭,但没有明显的肾结石疾病。

IF 2.3 4区 医学 Q2 UROLOGY & NEPHROLOGY Nephron Pub Date : 2024-01-01 Epub Date: 2024-03-25 DOI:10.1159/000536248
Pedro Lisboa Gonçalves, Hugo Diniz, Isabel Tavares, Sofia Dória, Juan Dong, McKenna Kyriss, Lynette Fairbanks, João Paulo Oliveira
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引用次数: 0

摘要

遗传性黄嘌呤尿症(HXAN)是一种罕见的代谢性疾病,由黄嘌呤脱氢酶(XDH)或钼辅因子硫酸酶(MOCOS)基因突变引起,分别定义为 HXAN I 型和 II 型。高尿酸血症、高尿酸尿症、血浆和尿液中黄嘌呤含量异常高,导致黄嘌呤肾炎和黄嘌呤结晶在组织中沉积,是 HXAN 的代谢特征。迄今为止,已在 HXAN I 型患者中发现了几种 XDH 基因的致病变异,但与人类 XDH 基因全缺失相关的临床表型尚不清楚。在此,我们报告了一例被诊断为 HXAN 的女性患者,其分子基因检测结果显示其 XDH 基因存在同卵微缺失。她病史的显著特点是:22 岁时被诊断出动脉高血压和微量白蛋白尿;25 岁时单胎妊娠,并在第三孕期出现蛋白尿和一过性肾功能恶化;妊娠期间意外发现不明原因的严重低尿酸血症;由于原发性无乳症而无法给新生女儿哺乳;35 岁时被诊断出慢性肾脏病 (CKD) 3 期;并在随后的 12 年中发展为终末期肾脏病。非侵入性实验室和影像学检查无法提供有关 CKD 病因的信息。这是首次描述与人类 XDH 基因自然敲除相关的临床表型。尽管缺乏肾脏组织病理学数据,但与同类鼠类模型所表现出的表型惊人的相似,验证了鼠类模型是人类疾病发病机理研究的有用来源,支持了黄嘌呤脱氢酶活性缺失可能代表慢性肾小管间质性肾炎易感因素的假设,即使在没有肾结石的患者中也是如此。
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Kidney Failure Secondary to Hereditary Xanthinuria due to a Homozygous Deletion of the XDH Gene in the Absence of Overt Kidney Stone Disease.

Hereditary xanthinuria (HXAN) is a rare metabolic disorder that results from mutations in either the xanthine dehydrogenase (XDH) or the molybdenum cofactor sulfurase genes (MOCOS), respectively defining HXAN type I and type II. Hypouricemia, hypouricosuria, and abnormally high plasma and urine levels of xanthine, causing susceptibility to xanthine nephrolithiasis and deposition of xanthine crystals in tissues, are the metabolic hallmarks of HXAN. Several pathogenic variants in the XDH gene have so far been identified in patients with HXAN type I, but the clinical phenotype associated with the whole deletion of the human XDH gene is unknown. Herein, we report the case of a woman diagnosed with HXAN, whose molecular genetic testing revealed a homozygous microdeletion involving the XDH gene. Distinctive features of her medical history were the diagnosis of arterial hypertension and microalbuminuria at 22 years of age; a single pregnancy at the age of 25, complicated by proteinuria and transient kidney function deterioration in the third trimester; unexplained severe hypouricemia incidentally discovered during pregnancy; inability to breastfeed her newborn daughter due to primary agalactia; chronic kidney disease (CKD) stage 3 diagnosed at age 35; and progression to end-stage kidney disease over the next 12 years. Protocol noninvasive laboratory and imaging investigation was not informative as to the cause of CKD. This is the first description of the clinical phenotype associated with a natural knockout of the human XDH gene. Despite the lack of kidney histopathology data, the striking similarities with the phenotypes exhibited by comparable murine models validate the latter as useful sources of mechanistic insights for the pathogenesis of the human disease, supporting the hypothesis that the absence of xanthine dehydrogenase activity might represent a susceptibility factor for chronic tubulointerstitial nephritis, even in patients without kidney stones.

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来源期刊
Nephron
Nephron UROLOGY & NEPHROLOGY-
CiteScore
5.00
自引率
0.00%
发文量
80
期刊介绍: ''Nephron'' comprises three sections, which are each under the editorship of internationally recognized leaders and served by specialized Associate Editors. Apart from high-quality original research, ''Nephron'' publishes invited reviews/minireviews on up-to-date topics. Papers undergo an innovative and transparent peer review process encompassing a Presentation Report which assesses and summarizes the presentation of the paper in an unbiased and standardized way.
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